| Literature DB >> 22622422 |
Manuela Pigors1, Dimitra Kiritsi1, Cristina Cobzaru1, Agnes Schwieger-Briel1, Jose Suárez2, Flavio Faletra3, Heikki Aho4, Leeni Mäkelä5, Johannes S Kern1, Leena Bruckner-Tuderman6, Cristina Has7.
Abstract
Acral peeling skin syndrome (APSS) is an autosomal recessive skin disorder characterized by acral blistering and peeling of the outermost layers of the epidermis. It is caused by mutations in the gene for transglutaminase 5, TGM5. Here, we report on clinical and molecular findings in 11 patients and extend the TGM5 mutation database by four, to our knowledge, previously unreported mutations: p.M1T, p.L41P, p.L214CfsX15, and p.S604IfsX9. The recurrent mutation p.G113C was found in 9 patients, but also in 3 of 100 control individuals in a heterozygous state, indicating that APSS might be more widespread than hitherto expected. Using quantitative real-time PCR, immunoblotting, and immunofluorescence analysis, we demonstrate that expression and distribution of several epidermal differentiation markers and corneodesmosin (CDSN) is altered in APSS keratinocytes and skin. Although the expression of transglutaminases 1 and 3 was not changed, we found an upregulation of keratin 1, keratin 10, involucrin, loricrin, and CDSN, probably as compensatory mechanisms for stabilization of the epidermal barrier. Our results give insights into the consequences of TGM5 mutations on terminal epidermal differentiation.Entities:
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Year: 2012 PMID: 22622422 DOI: 10.1038/jid.2012.166
Source DB: PubMed Journal: J Invest Dermatol ISSN: 0022-202X Impact factor: 8.551